Background

23Na magnetic resonance imaging (23Na-MRI) is able to measure Na+ in vivo in humans and allows quantification of tissue sodium distribution. We now tested the utility of 23Na-MRI technique in detecting and assessing sports-related acute muscular injury.

23Na magnetic resonance imaging (MRI) is a novel technique that allows in vivo quantification of tissue Na+ distribution. We developed this tool to investigate primary and secondary hypertension, changes in body and serum Na+ concentrations and Na+ shifts in patients undergoing dialysis (Kopp et al. 2013, 2012a, b). Others have developed similar techniques to inspect Na+ abnormalities in skeletal muscle diseases (Lehmann-Horn et al. 2012; Weber et al. 2011). Sports-related trauma leads to acute muscle injury that is oftentimes not easy to assess clinically. Conventional 1H-MRI can be helpful in detecting edema and structural changes. We were interested whether or not 23Na-MRI could also have utility in detecting and quantitatively assessing sports-related injury.

A 35 year-old woman presented with acute sharp pain in her left calf. The pain suddenly appeared during a volley ball game. The patient could not recall any trauma. There was pain with walking and on the next day she noted swelling of the affected area. The physical examination was otherwise entirely normal. Arterial blood supply and venous drainage of the left lower leg were unremarkable. There was no indication of fracture and neurologically, the extremity was intact. We suspected torn fibers in the triceps surae and prescribed cooling and elevation of the injured lower leg.

We performed 23Na- and 1H-MR imaging with a 3 Tesla scanner (Magnetom Trio, Siemens Healthcare GmbH, Erlangen, Germany) of both lower legs. We used a customized 23Na knee coil as described previously (Kopp et al. 2013, 2012a, b; Hammon et al. 2015a, b). A gradient echo 23Na sequence was applied (total acquisition time TA: 3.25 min, echo time TE: 2.07 ms, repetition time TR: 100 ms, flip angle FA: 90°, 32 averages, resolution: 3 × 3 × 30 mm3). We additionally performed a T1-weighted fast-low-angle-shot (FLASH)-sequence for anatomic information. The scanning protocol is shown in Table 1. To calibrate Na+ signals, calibration tubes with 10, 20, 30 and 40 mmol/l NaCl were arranged below both calf muscles. Gray-scale measurements of the tubes served as calibration standards for 23Na-MRI by relating intensity to a concentration in a linear trend analysis. We calibrated these techniques in earlier studies. Amputated lower limbs from subjects undergoing operations because of malignancy or diabetes were measured with 23Na-MRI. These limbs were desiccated (the difference between wet weight and dry weight was considered tissue water content) and ashed and measured with atomic absorption spectrometry, allowing us to show a very close correlation between 23Na-MRI signal and actual Na+ concentrations in muscle and skin (Kopp et al. 2013; Dahlmann et al. 2015).

Table 1

Scanning protocol

Localizer

T1-weighted fast-low-angle-shot (FLASH)-sequence

Gradient echo 23Na sequence (acquired 4 times successively)

Total acquisition time (TA; min)

0.15

2.08

3.25

Echo time (TE; ms)

4

2.46

2.07

Repetition time (TR; ms)

8.6

250

100

Flip angle (FA; °)

20

60

90

Averages

2

2

32

Bandwidth (Hz/pixel)

320

310

430

Field of view (FoV; mm)

192

192

192

Matrix (pixel)

256

256

64

Resolution (mm)

0.75 × 0.75 × 10

0.75 × 0.75 × 5

3 × 3 × 30

In the conventional T1 weighted 1H image (Fig. 1, left), all anatomic compartments can be seen in detail, while all Na+ calibration tubes appear at a similar intensity. The affected left lower leg presented a discrete swelling of the subcutaneous region in comparison to the contralateral leg. Muscle tissue itself seemed not to be affected and there is no sign of hemorrhagic bleeding. The concomitant 23Na-MRI showed a strong hyperintense signal in the affected leg region (Fig. 1, right), indicating increased local Na+ concentration. There was a 2.4-fold increase in Na+ concentration in the half-moon shaped region containing the medial left triceps surae muscle and adjacent tissue, compared to the corresponding soft tissue of the contralateral non-affected leg (Na+ 43.5 vs. 18.0 mmol/l). The hyperintense region was separated from the neighboring regions by manual outlining by a radiologist. The same region was used in the follow-up signal measurements.

Fig. 1

1H-MR imaging [T1-weighted fast-low-angle-shot (FLASH)-sequence, left] and 23Na-MR imaging (right) of both lower legs immediately after injury. The left leg shows a half-moon shaped, hyperintense Na+ rich area on the medial side (arrow). Highest muscle Na+ signal could be found in the region of the left medial gastrocnemius muscle (there was a 2.4-fold increase in Na+ concentration compared to the corresponding soft tissue of the contralateral non-affected leg, 43.5 vs. 18.0 mmol/l). The calibration tubes below the lower legs contain 10, 20, 30 and 40 mmol/l NaCl. Gray-scale measurements of the tubes served as calibration standards for 23Na-MRI by relating intensity to a concentration in a linear trend analysis

1H-MR imaging [T1-weighted fast-low-angle-shot (FLASH)-sequence, left] and 23Na-MR imaging (right) of both lower legs 2 weeks after injury. The area of hyperintense Na+ rich tissue was reduced, but could still be clearly visualized at the level of the left medial gastrocnemius muscle (arrow, Na+ concentration compared to the corresponding soft tissue of the contralateral non-affected leg: 37.5 vs. 18.5 mmol/l). Muscle function of the leg was completely restored by this point

Based on our measurements, we assume that muscle fibers of the left medial gastrocnemius were torn, as the highest Na+ concentration was found in this region. Moreover, Na+ elevation in this muscle might not only be based on edema, but also on disrupted membrane potential with subsequent intracellular Na+ influx. 23Na-MRI examinations with protocols that can differentiate between intra and extracellular Na+ could be developed to address this notion further. Other investigators have used 23Na-MR imaging to study Na+ accumulation in patients with Duchenne’s muscular dystrophy and even to test the value of eplerenone treatment for this condition (Lehmann-Horn et al. 2012; Weber et al. 2011).

Our patient happened to have an injury that could easily be investigated with the coil we developed for our studies on Na+ metabolism. However, surface coils and coils of other configurations could be developed to study the upper leg, shoulder, back and other body components. Such tools could have utility in quantitatively assessing sports-related injuries and also responses to treatments. They could help in establishing restitutio ad integrum and thereby assist physicians in determining when players can safely return to the field.

Authors’ contributions

All authors have made substantial contributions to conception and design, or acquisition of data, or analysis and interpretation of data; MH, AD, CK, PL, FCL and JT have been involved in drafting the manuscript or revising it critically for important intellectual content; all authors have given final approval of the version to be published; and all authors agree to be accountable for all aspects of the work in ensuring that questions related to the accuracy or integrity of any part of the work are appropriately investigated and resolved. All authors read and approved the final manuscript.

Acknowledgements

The authors have nothing to disclose. A Grant from the Interdisciplinary Center for Clinical Research, Erlangen (IZKF) to J.T., and a Grant from the IZKF, Erlangen to C.K. supported the study. We thank Daniela Amslinger for her assistance in analyzing the MR images.

Competing interests

The authors declare that they have no competing interests.

Ethics approval and consent to participate

The University of Erlangen Committee on Human Subjects (Ethics committee) reviewed and approved this study (Re.-No. 3948). Written informed consent was obtained from our participant.

Funding

The study was supported by a Grant from the Interdisciplinary Center for Clinical Research, Erlangen (IZKF).

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